Identifying these gene variants may allow researchers to prevent a deadly complication of coronary stent implantation in people with coronary artery disease.

New York

– October 26, 2011 /Press Release/ ––

In a first-of-its-kind study, researchers from Mount Sinai School of Medicine have discovered several gene variants contributing to early stent thrombosis (ST), a devastating and often deadly complication after coronary stent implantation in people with coronary artery disease. The team found that three of these variants were associated with impaired sensitivity to the common blood thinner clopidogrel, and a fourth that affects a blood platelet receptor involved in platelet aggregation and clot formation. Analyzing these gene variants will help researchers identify patients at risk for early stent thrombosis and take measures to prevent it. The data also provide a clinical and genomic score that indicates the best predictive accuracy for stent thrombosis risk. The findings are published in the October 26 issue of the Journal of the American Medical Association.

Through a partnership with the Institut de Cardiologie at Pitié-Salpêtrière University Hospital in Paris, France, the research team evaluated the DNA of 123 patients who had undergone stent implantation and developed early ST while treated with dual antiplatelet therapy, which is a combination of aspirin and clopidogrel. The patient information was shared as part of ONline ASSIstance for Stent Thrombosis (ONASSIST), a nationwide web registry of patients in France. Looking at 23 genetic variants previously associated with clopidogrel metabolism, platelet receptor function, and the control of blood clotting, they found four that were predictive risk factors of early ST. They also found that a low dose of clopidogrel in combination with a proton pump inhibitor, which is a drug to treat acid reflux, also increased the risk of early ST.

"Our research indicates that early stent thrombosis is strongly related to ineffectiveness of clopidogrel in certain patients," said Jean-Sebastien Hulot, MD, PhD, Associate Professor of Medicine in the Division of Cardiology and Director Pharmacogenomics and Personalized Therapeutics at the Cardiovascular Research Center at Mount Sinai School of Medicine. "Now that we have a clearer understanding of the mechanism behind the development of stent thrombosis, we can take preventive measures to protect our patients from this deadly complication."

The research team compared the genetic code of people registered in the ONASSIST program with 246 coronary patients without early ST. They evaluated alleles, which are types of genetic variation that arise from mutations, of 23 genes. They found that CYP2C19*2 allele, which is commonly associated with loss of enzyme function, was highly prevalent in people presenting with early ST, as was the allele ABCB1 3435T, and both were infrequent in the control group. Two other alleles, CYP2C19*17 and ITGB3, were prevalent in the healthy control group but not in the early ST group indicating a protective effect. The scientists developed a genetic score where the more of these mutations that the patient had, the higher their risk for developing early ST. This risk was independent of clinical risk factors, including the use of proton pump inhibitors, acuteness of PCI, complexity of cardiac lesions, left ventricular heart function, and a high dose of clopidogrel. Only two of these risk factors – clopidogrel dose and proton pump inhibitor use – are modifiable in reducing risk for early ST. Eventually, the best prediction was achieved using the combination of both clinical and genetic factors. The authors conclude that this "clinico-genomic" approach could be useful prior to stent implantation to identify the patients with high-ST risk.

"We found that, independent of other clinical risk factors, these genetic factors play a critical role in the development of early ST," said Dr. Hulot. "Altogether, our data will help clinicians understand the factors contributing to early ST, and allow them to reduce the outcome risk to these patients. Understanding the genetic factors provides researchers with new drug targets for future study to reduce the genetic risk as well."

Mount Sinai's Cardiovascular Research Center plans to continue the partnership with the Institut de Cardiologie at Pitié-Salpêtrière University Hospital in Paris to develop an international cardiogenomic laboratory to better understand genetic risk factors associated with heart disease and treatments for heart disease to improve and better target clinical care for patients.

PCI is a minimally invasive technique used to treat patients with diseased coronary arteries caused by a buildup of plaque and cholesterol. During the procedure, a catheter is threaded through the body, typically from an artery in the groin to a blocked or occluded vessel in the heart. The occlusion is removed and a stent is often inserted to maintain flow within the blood vessel. Up to four percent of patients undergoing PCI experience early ST, which is deadly in 40 percent of those patients.

About The Mount Sinai Medical Center

The Mount Sinai Medical Center encompasses both The Mount Sinai Hospital and Mount Sinai School of Medicine. Established in 1968, Mount Sinai School of Medicine is one of the leading medical schools in the United States. The Medical School is noted for innovation in education, biomedical research, clinical care delivery, and local and global community service. It has more than 3,400 faculty in 32 departments and 14 research institutes, and ranks among the top 20 medical schools both in National Institutes of Health (NIH) funding and by US News and World Report.

The Mount Sinai Hospital, founded in 1852, is a 1,171-bed tertiary- and quaternary-care teaching facility and one of the nation’s oldest, largest and most-respected voluntary hospitals. In 2011, US News and World Report ranked The Mount Sinai Hospital 16th on its elite Honor Roll of the nation’s top hospitals based on reputation, safety, and other patient-care factors. Of the top 20 hospitals in the United States, Mount Sinai is one of 12 integrated academic medical centers whose medical school ranks among the top 20 in NIH funding and US News & World Report and whose hospital is on the US News and World Report Honor Roll. Nearly 60,000 people were treated at Mount Sinai as inpatients last year, and approximately 560,000 outpatient visits took place.